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人肺发育中呼吸上皮内表面活性蛋白B和表面活性蛋白C的时空分布及mRNA表达

Temporal-spatial distribution of SP-B and SP-C proteins and mRNAs in developing respiratory epithelium of human lung.

作者信息

Khoor A, Stahlman M T, Gray M E, Whitsett J A

机构信息

Department of Pediatrics, Vanderbilt University, Nashville, Tennessee 37232-2370.

出版信息

J Histochem Cytochem. 1994 Sep;42(9):1187-99. doi: 10.1177/42.9.8064126.

Abstract

We determined the temporal and spatial distribution of surfactant protein B (pro-SP-B) and C (pro-SP-C) mRNAs and proteins by immunohistochemistry and in situ hybridization in fetal, neonatal, and adult human lung. Pro-SP-B and SP-B mRNA were detected in bronchi and bronchioles by 15 weeks' gestation. After 25 weeks, pro-SP-B, active SP-B peptide, and SP-B mRNA were co-localized in bronchiolo-alveolar portal cells and in Type II epithelial cells. In adult lung, pro-SP-B and SP-B mRNA were detected primarily in non-ciliated bronchiolar epithelial cells and in Type II cells in the alveolus. Pro-SP-C and SP-C mRNA were detected in cells lining terminal airways from 15 weeks' gestation and thereafter. After 25 weeks, SP-C mRNA and precursor protein were detected in epithelial cells of the bronchiolo-alveolar portals and in Type II cells, where expression increased with advancing gestational age. Distinct cellular patterns of staining for pro-SP-B compared with SP-B active peptide support the concept that its proteolytic processing or cellular routing may be influenced by cell type and/or cell differentiation. SP-B and SP-C are expressed primarily in distal conducting and terminal airway epithelium of human fetal lung well in advance of surfactant lipid synthesis or physiologic requirements to produce pulmonary surfactant at the time of birth.

摘要

我们通过免疫组织化学和原位杂交技术,确定了表面活性蛋白B(pro-SP-B)和C(pro-SP-C)的mRNA及蛋白在人胎儿、新生儿和成人肺组织中的时空分布。妊娠15周时,在支气管和细支气管中检测到pro-SP-B和SP-B mRNA。25周后,pro-SP-B、活性SP-B肽和SP-B mRNA在细支气管肺泡门细胞和II型上皮细胞中共定位。在成人肺组织中,pro-SP-B和SP-B mRNA主要在无纤毛细支气管上皮细胞和肺泡II型细胞中检测到。妊娠15周及之后,在终末气道内衬细胞中检测到pro-SP-C和SP-C mRNA。25周后,在细支气管肺泡门的上皮细胞和II型细胞中检测到SP-C mRNA和前体蛋白,其表达随胎龄增加而增加。与SP-B活性肽相比,pro-SP-B染色的不同细胞模式支持这样的概念,即其蛋白水解加工或细胞转运可能受细胞类型和/或细胞分化的影响。在出生时产生肺表面活性物质所需的表面活性脂质合成或生理需求之前,SP-B和SP-C主要在人胎儿肺的远端传导和终末气道上皮中表达。

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